Luo J, Balkin N, Stewart J F, Sarwark J F, Charrow J, Nye J S
Department of Molecular Pharmacology and Biological Chemistry, Northwestern University, Chicago, Illinois 60611, USA.
Am J Med Genet. 2000 Mar 20;91(3):227-30. doi: 10.1002/(sici)1096-8628(20000320)91:3<227::aid-ajmg14>3.0.co;2-i.
Neural tube defects (NTD) are common findings in the 13q deletion syndrome, but the relationship between the 13q- syndrome and NTDs is poorly understood. We present a child with a 13q deletion and lumbosacral myelomeningocele. This was a boy with microcephaly, telecanthus, minor facial anomalies, and ambiguous genitalia. Cytogenetic and fluorescence in situ hybridization analysis showed a de novo 46,XY,del(13)(q33.2-->qter) with no visible translocation. By using microsatellite markers, the deletion breakpoint was mapped to a 350-kb region between D13S274 and D13S1311 and was paternal in origin. An analysis of 13q deletions with NTDs, including the present case, suggests that a deletion in 13q33-34 is sufficient to cause an NTD. The deletions associated with NTDs are distal to and nonoverlapping with the previously defined critical region in 13q32 for the major malformation syndrome [Brown et al., 1999: Am J Hum Genet 57: 859-866]. Our analysis also suggests that one or more genes in 13q33-34 produces NTDs by haploinsufficiency.
神经管缺陷(NTD)是13q缺失综合征中的常见表现,但13q缺失综合征与NTD之间的关系尚不清楚。我们报告一名患有13q缺失和腰骶部脊髓脊膜膨出的儿童。这是一名男孩,有小头畸形、眼距过宽、轻微面部异常和生殖器模糊。细胞遗传学和荧光原位杂交分析显示为新发的46,XY,del(13)(q33.2→qter),无可见易位。通过使用微卫星标记,缺失断点定位于D13S274和D13S1311之间的一个350kb区域,且起源于父方。对包括本病例在内的伴有NTD的13q缺失的分析表明,13q33 - 34的缺失足以导致NTD。与NTD相关的缺失位于13q32中先前定义的主要畸形综合征关键区域的远端且不与之重叠[Brown等人,1999年:《美国人类遗传学杂志》57:859 - 866]。我们的分析还表明,13q33 - 34中的一个或多个基因通过单倍剂量不足导致NTD。
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